p-Nitrophenylcarbonyl-PEG-PE-liposomes: fast and simple attachment of specific ligands, including monoclonal antibodies, to distal ends of PEG chains via p-nitrophenylcarbonyl groups

Torchilin, Vladimir P.; Levchenko, Tatyana; Lukyanov, Anatoly N.; Khaw, Ban‐An; Klibanov, A.L.; Rammohan, Ram; Samokhin, Gennady P.; Whiteman, Kathleen R.

doi:10.1016/s0005-2728(01)00165-7

Cited by 255 publications

(195 citation statements)

References 43 publications

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“…Monoclonal antibody (mAb) 2G4 was produced and purified in our laboratory. Also, pNP-PEG 3400 -PE was synthesized and purified according to an established method in our laboratory (27) Developing the method of coupling oxidized antibody to the PEG terminus through a hydrazone bond as suggested by Hansen et al (28), we devised our own scheme of conjugate reaction for synthesis of pH-cleavable PEG-PE. The reaction was performed in two steps: first, the activation of mPEG 2000 -CHO with PDPH, and second, the conjugation of 1,2-dipalmitoylsn-glycero-3-phosphothioethanol (sodium salt) (PE-SH) to activated mPEG-CHO.…”

Section: Methodsmentioning

confidence: 99%

“SMART” Drug Delivery Systems: Double-Targeted pH-Responsive Pharmaceutical Nanocarriers

et al. 2006

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In order to develop targeted pharmaceutical carriers additionally capable of responding certain local stimuli, such as decreased pH values in tumors or infarcts, targeted long-circulating PEGylated liposomes and PEG-phosphatidylethanolamine (PEG-PE)-based micelles have been prepared with several functions. First, they are capable of targeting a specific cell or organ by attaching the monoclonal antimyosin antibody 2G4 to their surface via pNP-PEG-PE moieties. Second, these liposomes and micelles were additionally modified with biotin or TAT peptide (TATp) moieties attached to the surface of the nanocarrier by using biotin-PE or TATp-PE or TATp-short PEG-PE derivatives. PEG-PE used for liposome surface modification or for micelle preparation was made degradable by inserting the pH-sensitive hydrazone bond between PEG and PE (PEG-Hz-PE). Under normal pH values, biotin and TATp functions on the surface of nanocarriers were "shielded" by long protecting PEG chains (pH-degradable PEG 2000 -PE or PEG 5000 -PE) or by even longer pNP-PEG-PE moieties used to attach antibodies to the nanocarrier (non-pH-degradable PEG 3400 -PE or PEG 5000 -PE). At pH 7.5-8.0, both liposomes and micelles demonstrated high specific binding with 2G4 antibody substrate, myosin, but very limited binding on an avidin column (biotin-containing nanocarriers) or internalization by NIH/3T3 or U-87 cells (TATp-containing nanocarriers). However, upon brief incubation (15-to-30 min) at lower pH values (pH 5.0-6.0) nanocarriers lost their protective PEG shell because of acidic hydrolysis of PEG-Hz-PE and acquired the ability to become strongly retained on avidin-column (biotin-containing nanocarriers) or effectively internalized by cells via TATp moieties (TATp-containing nanocarriers). We consider this result as the first step in the development of multifunctional stimuli-sensitive pharmaceutical nanocarriers.

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Section: Methodsmentioning

confidence: 99%

“SMART” Drug Delivery Systems: Double-Targeted pH-Responsive Pharmaceutical Nanocarriers

et al. 2006

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“…The reaction of HP-$-CD-PLA-pNP and DPPE as reported previously, 33 is performed with with slight modification. Briefly, 1.0 g of HP-$-CD-PLA-pNP was dissolved in 3 mL of chloroform.…”

Section: Synthesis Of Hp-β-cd-pla-dppe Copolymersmentioning

confidence: 99%

“…Firstly, the inclusion complexes may be formed from the accessible residues of DOX with the hydrophobic cavity of HP-$-CD moiety, because such inclusion complexes were easily formed from small organic molecules with free HP-$-CD. 33 The cavity size of HP-$-CD is suitable to bind DOX. Therefore, the formation of inclusion complexes was quite possible.…”

Section: Formation Of Dox-loaded Nanoparticlesmentioning

confidence: 99%

Hydroxypropyl-β-Cyclodextrin Copolymers and Their Nanoparticles as Doxorubicin Delivery System

Wang

Zhang

Liang

et al. 2011

Journal of Pharmaceutical Sciences

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“…pNP-PEG-PE was synthesized according to a procedure published by us (45). Briefly, 0.1 mmol of PE was dispersed in 8 ml of chloroform supplemented with 2 ml of triethylamine.…”

mentioning

confidence: 99%

Cell transfection in vitro and in vivo with nontoxic TAT peptide-liposome–DNA complexes

Torchilin

Levchenko

Rammohan

et al. 2003

Proc. Natl. Acad. Sci. U.S.A.

419

255

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p-Nitrophenylcarbonyl-PEG-PE-liposomes: fast and simple attachment of specific ligands, including monoclonal antibodies, to distal ends of PEG chains via p-nitrophenylcarbonyl groups

Cited by 255 publications

References 43 publications

“SMART” Drug Delivery Systems: Double-Targeted pH-Responsive Pharmaceutical Nanocarriers

“SMART” Drug Delivery Systems: Double-Targeted pH-Responsive Pharmaceutical Nanocarriers

Hydroxypropyl-β-Cyclodextrin Copolymers and Their Nanoparticles as Doxorubicin Delivery System

Cell transfection in vitro and in vivo with nontoxic TAT peptide-liposome–DNA complexes

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